ATR/ATM Targets Are Phosphorylated by ATR in Response to Hypoxia and ATM in Response to Reoxygenation
The ATR kinase phosphorylates both p53 and Chk1 in response to extreme hypoxia (oxygen concentrations of less than 0.02%). In contrast to ATR, loss of ATM does not affect the phosphorylation of these or other targets in response to hypoxia. However, hypoxia within tumors is often transient and is in...
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Veröffentlicht in: | The Journal of biological chemistry 2003-04, Vol.278 (14), p.12207-12213 |
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Sprache: | eng |
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Zusammenfassung: | The ATR kinase phosphorylates both p53 and Chk1 in response to extreme hypoxia (oxygen concentrations of less than 0.02%).
In contrast to ATR, loss of ATM does not affect the phosphorylation of these or other targets in response to hypoxia. However,
hypoxia within tumors is often transient and is inevitably followed by reoxygenation. We hypothesized that ATR activity is
induced under hypoxic conditions because of growth arrest and ATM activity increases in response to the oxidative stress of
reoxygenation. Using the comet assay to detect DNA damage, we find that reoxygenation induced significant amounts of DNA damage.
Two ATR/ATM targets, p53 serine 15 and histone H2AX, were both phosphorylated in response to hypoxia in an ATR-dependent manner.
These phosphorylations were then maintained in response to reoxygenation-induced DNA damage in an ATM-dependent manner. The
reoxygenation-induced p53 serine 15 phosphorylation was inhibited by the addition of N -acetyl- l -cysteine (NAC), indicating that free radical-induced DNA damage was mediated by reactive oxygen species. Taken together these
data implicate both ATR and ATM as critical roles in the response of hypoxia and reperfusion in solid tumors. |
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ISSN: | 0021-9258 1083-351X |
DOI: | 10.1074/jbc.M212360200 |